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Parisons between 68181-17-9 site groups. OS was defined as described previously [15]. Prognostic significance was assessed using Kaplan-Meier survival estimates and log-rank tests. Cox’s proportional hazards regression model was used to analyze the independent prognostic factors. All tests were two-tailed and p,0.05 was considered statistically significant.Results CD151 is Overexpressed in HGCCD151 expression was analyzed by RT-PCR and immunoblotting in HGC tumor and matched nontumor tissues. CD151 was expressed at low levels in nontumor tissues compared with HGC tissues. As shown in Fig. 1A,B and C, the relative expression of the CD151 protein in HGC samples was 2.9560.21 (range, 1.13 2 3.59) compared to 1.3060.09 (range, 1.0021.81) in nontumor samples, and the difference was statistically significant (p,0.01). Furthermore, CD151 expression levels were significantly lower in HGEC than in HGC-27, AGS, MKN28 and MGC803 cells (p,0.05). No differences in CD151 expression levels were detected among HGC cells 25331948 (Fig. 1D, E and F). Immunohistochemstry (IHC) analyses confirmed that the CD151 protein was expressed at higher levels in HGC tissues than in matched nontumor tissues (Fig. 1G).Expression of CD151 or Integrin a3 is Positively Associated with Malignant Phenotypes of 15900046 HGC by ImmunohistochemistryThe expression of CD151 and integrin a3 protein was investigated in 76 primary HGC patients using tissue microarrays(TMA). CD151 protein immunoreactivity localized to the cell membrane (Fig. 4A). In tumor tissues, CD151 expression showed considerable heterogeneity in the different samples (Figs. 4a1, b1, c1 and d1). CD151high accounted for 50 (38/76) of the whole cohort. As shown in Table 1, CD151high was significantly correlated with tumor size (p = 0.021), depth of invasion (p = 0.004), lymph node 115103-85-0 site involvement (p = 0.028) and high tumor stage (p = 0.002). However, other clinical characteristics, including age, sex and tumor differentiation, were not significantly related to the expression of CD151. The membranes of tumor cells stained positive for integrin a3 (Figs. 4a2, b2, c2, and d2). In all the tissues analyzed, high levels of integrin a3 expression were detected in 27 HGC tissue samples (35.52 ). Consistent with the results of previous studies [16,18], patients with high integrin a3 expression were more likely to exhibit aggressive features. Integrin a3high patients showed larger tumors (p = 3.46E24), greater depth of invasion (p = 0.001), higher tumor stage (p = 0.005), and more lymph node involvement (p = 0.040) than patients with low integrin a3 expression (Table 1).CD151 Promoted the Invasion and Metastasis of HGC Cells in vitro and in vivoTo examine the role of CD151 in HGC cells, we modified the expression of CD151 in HGC-27 cells by RNA interference and cDNA-CD151 transfection (Fig. 2A). The results of the wound healing assay showed a delay in the wound closure rate of shRNACD151-HGC-27 cells at 48 h compared with HGC-27-Mock cells, which was recovered by cDNA-CD151 transfection (Fig. 2B). Down-regulation of CD151 had no significant effect on cell proliferation (p.0.05, Fig. 2C). However, the downregulation of CD151 expression impaired the invasiveness of HGC27 cells (Figs. 2D, E). To further explore the role of CD151 in tumor metastasis in vivo, MGC-803-Mock, MGC-803-vshRNACD151 and MGC803-vshRNACD151-cDNA-CD151 cells were transplanted into nude mice through the lateral tail vein. Histologic analysis of the lungs of mice confirmed that the down-regul.Parisons between groups. OS was defined as described previously [15]. Prognostic significance was assessed using Kaplan-Meier survival estimates and log-rank tests. Cox’s proportional hazards regression model was used to analyze the independent prognostic factors. All tests were two-tailed and p,0.05 was considered statistically significant.Results CD151 is Overexpressed in HGCCD151 expression was analyzed by RT-PCR and immunoblotting in HGC tumor and matched nontumor tissues. CD151 was expressed at low levels in nontumor tissues compared with HGC tissues. As shown in Fig. 1A,B and C, the relative expression of the CD151 protein in HGC samples was 2.9560.21 (range, 1.13 2 3.59) compared to 1.3060.09 (range, 1.0021.81) in nontumor samples, and the difference was statistically significant (p,0.01). Furthermore, CD151 expression levels were significantly lower in HGEC than in HGC-27, AGS, MKN28 and MGC803 cells (p,0.05). No differences in CD151 expression levels were detected among HGC cells 25331948 (Fig. 1D, E and F). Immunohistochemstry (IHC) analyses confirmed that the CD151 protein was expressed at higher levels in HGC tissues than in matched nontumor tissues (Fig. 1G).Expression of CD151 or Integrin a3 is Positively Associated with Malignant Phenotypes of 15900046 HGC by ImmunohistochemistryThe expression of CD151 and integrin a3 protein was investigated in 76 primary HGC patients using tissue microarrays(TMA). CD151 protein immunoreactivity localized to the cell membrane (Fig. 4A). In tumor tissues, CD151 expression showed considerable heterogeneity in the different samples (Figs. 4a1, b1, c1 and d1). CD151high accounted for 50 (38/76) of the whole cohort. As shown in Table 1, CD151high was significantly correlated with tumor size (p = 0.021), depth of invasion (p = 0.004), lymph node involvement (p = 0.028) and high tumor stage (p = 0.002). However, other clinical characteristics, including age, sex and tumor differentiation, were not significantly related to the expression of CD151. The membranes of tumor cells stained positive for integrin a3 (Figs. 4a2, b2, c2, and d2). In all the tissues analyzed, high levels of integrin a3 expression were detected in 27 HGC tissue samples (35.52 ). Consistent with the results of previous studies [16,18], patients with high integrin a3 expression were more likely to exhibit aggressive features. Integrin a3high patients showed larger tumors (p = 3.46E24), greater depth of invasion (p = 0.001), higher tumor stage (p = 0.005), and more lymph node involvement (p = 0.040) than patients with low integrin a3 expression (Table 1).CD151 Promoted the Invasion and Metastasis of HGC Cells in vitro and in vivoTo examine the role of CD151 in HGC cells, we modified the expression of CD151 in HGC-27 cells by RNA interference and cDNA-CD151 transfection (Fig. 2A). The results of the wound healing assay showed a delay in the wound closure rate of shRNACD151-HGC-27 cells at 48 h compared with HGC-27-Mock cells, which was recovered by cDNA-CD151 transfection (Fig. 2B). Down-regulation of CD151 had no significant effect on cell proliferation (p.0.05, Fig. 2C). However, the downregulation of CD151 expression impaired the invasiveness of HGC27 cells (Figs. 2D, E). To further explore the role of CD151 in tumor metastasis in vivo, MGC-803-Mock, MGC-803-vshRNACD151 and MGC803-vshRNACD151-cDNA-CD151 cells were transplanted into nude mice through the lateral tail vein. Histologic analysis of the lungs of mice confirmed that the down-regul.

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